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A PROJECT ON A FED VS FASTED STATE SUPERVISOR; SUBMITTED BY; Dr. SUNIL KUMAR JAIN DIVYA JAISWAL M PHARM, Ph.D M PHARM(PHARMACEUTICS) (PHARMACEUTICS) 2ND SEM, DEPARTMENT OF DEPARTMENT OF PHARMACY GGV BILASPUR PHARMACY GGV BILASPUR
CONTENT 1. INTRODUCTION 2. FED STATE METABOLISM a) insulin independent glucose uptake b) Insulin dependent glucose uptake 3. FASTED STATE METABOLISM a) Liver metabolism b) Red blood cell metabolism c) Brain metabolism d) Skeletal muscle metabolism e) Adipose metabolism 4. FED VS FASTED STATE 5. COCLUSION
INTRODUCTION • Intermittent Fasting (Time-Restricted Eating) Fed vs. Fasted Your body is designed to smoothly transition between two different and opposing states: ‘Fed’, and ‘Fasted’. • In the fed state, insulin is elevated, and this signals your body to store excess calories in your fat cells. In the presence of insulin, the burning of fat is halted, while the body burns glucose (from your last meal) instead. • In the fasted state, insulin is low (while glucagon and growth hormone, opposing hormones to insulin, are elevated). The body starts mobilizing stored body fat from your fat cells and burning this fat for energy (instead of glucose). • FED STATE refers to the period following a meal and is characterized by levels of nutrients in the blood. There are high circulating levels of a family of simple sugar was most important being glucose. • FASTED STATE: it means exercising after having not eaten for several hours typically early in the morning when your last meal was dinner. • Glucose homeostasis is fundamental to the human body and regulated primarily by the levels of four major hormones. 1insulin 2 glucagon 3 cortisol 4 epinephrine
FED STATE METABOILSM In the fed state, or postprandial, elevated glucose levels trigger the release of insulin from the pancreas. As insulin levels rise, there is an increase in glucose uptake, oxidation, and storage in peripheral tissues as well as increases in other anabolic pathways. Under these conditions, most tissues (liver, skeletal muscle, adipose, brain, and red blood cells) will increase glucose uptake and oxidation (table 1). Each tissue will take up glucose in the fed state using one of the glucose transporters (GLUT) known to facilitate glucose transport across the plasma membrane. This family of proteins can be broadly categorized as insulin- independent and insulin-dependent transporters. TABLE 1 SUMMARY TABLE OF FULES USED IN THE FED STATE Tissue type Fuel utilized in fed state Primary glucose transporter Liver Glucose GLUT2 (insulin-independent) Red blood cells Glucose GLUT1 (insulin-independent) Brain Glucose GLUT1 and GLUT3 (insulin- independent) Skeletal muscle Glucose GLUT4 (insulin-dependent) Adipose Glucose GLUT4 (insulin-dependent)
INSULIN INDEPENDENT GLUCOSE UPTAKE • The brain and red blood cells will always preferentially oxidize glucose regardless of hormone levels. Consequently, both tissues have a prevalence of GLUT1 transporters on the cell membrane. • GLUT1 is present on the blood brain barrier, while GLUT3 is predominant on the brain. • GLUT1 has a lower Km (higher affinity) for glucose, ensuring glucose transport to these important tissues. Likewise, glucose uptake in the liver is also insulin-independent and is facilitated by GLUT2 transporters. The pancreas also predominantly expresses GLUT1 and is able to take up glucose in this manner. • Red blood cell metabolism • The red blood cell lacks mitochondria, therefore it oxidizes glucose under both fed and fasted conditions. Glucose can be oxidized by: • Glycolysis. Glucose is oxidized to pyruvate and converted to lactate, which will enter the Cori Cycle. (Lactate is returned to the liver and used as a substrate for gluconeogenesis.) • Pentose phosphate pathway. Glucose is initially oxidized to ribulose 5-phosphate. In addition to the production of this 5-C sugar, more importantly NADPH is produced, which is needed as a reducing agent in the red blood cell
fig 1. overview of fed state
Brain metabolism The brain will preferentially oxidize glucose under most conditions with the exception of starvation states. Liver metabolism In the liver, glucose is taken up in an insulin-independent manner, and the activity of the following processes increased in the fed state are summarized in table 1and 2 1.Glycolysis. Glucose will be oxidized to pyruvate, which can enter the TCA cycle after conversion to acetyl-CoA . 2.Glycogen synthesis. Glucose 6-phosphate is used to synthesize glycogen. Pentose phosphate pathway. Glucose 6-phosphate can be used to generate five-carbon sugars and NADPH. 3.Tricarboxylic acid cycle. The TCA cycle will oxidize acetyl-CoA to generate NADH, FADH 2 , and GTP. The acetyl- CoA that enters the cycle is fully oxidized and released as CO2. 4.Cholesterol synthesis. Acetyl-CoA transported to the cytosol is used to synthesize cholesterol, which can be used for many cellular process. 5.Fatty acid synthesis. Excess citrate from the TCA cycle is shuttled out of the mitochondria and cleaved into oxaloacetate (OAA) and acetyl-CoA. The cytosolic acetyl-CoA can be used for fatty acid synthesis or cholesterol synthesis (section 4.4). Ultimately fatty acid synthesis leads to VLDL synthesis and secretion. 6.Urea cycle. Depending on diet and translation needs, excess amino acids will be deaminated through transamination reactions, and the nitrogen will enter the urea cycle as aspartate or free ammonia. Excess amino acids are not stored, rather the deaminated carbon skeletons can be stored as glycogen or triacylglycerol.
INSULIN DEPENDENT GLUCOSE UPTAKE • in contrast, the skeletal muscle and adipose tissues require insulin for glucose uptake. GLUT4 is the primary glucose transporter on these tissues, and in the absence of insulin this transporter is predominantly bound to intracellular vesicles. When the cell receives a signal (via insulin binding the insulin receptor), this cell signaling event allows the GLUT4 containing vesicles to fuse with the plasma membrane where it will facilitate glucose uptake. Skeletal muscle metabolism The skeletal muscle will increase uptake of both amino acids and glucose under fed conditions. Glycolysis. Glucose will be oxidized to pyruvate, which can enter the TCA cycle after conversion to acetyl-CoA. Protein synthesis. Amino acids will be used for protein synthesis (anabolic metabolism). Glycogen synthesis. Glucose 1-phosphate can be converted to UDP-glucose and stored as glycogen. Adipose metabolism In the adipose tissue, glucose as well as dietary fat and cholesterol (transported as chylomicrons; are taken up by the adipose tissue. Glucose has several potential fates described below, while dietary fat is stored as triacylglycerol. Glycolysis. Glucose can be oxidized to pyruvate which can enter the TCA cycle after conversion to acetyl-CoA. Pentose phosphate pathway. Glucose will be oxidized to generate NADPH needed for fatty acid synthesis. TAG synthesis. Oxidation of glucose to glycerol 3-phosphate is needed for the synthesis of triacylglycerols (TAGs).
Pathway Summary Regulatory enzyme Glycolysis Glucose oxidation to pyruvate Glucokinase/Hexokinase Phosphofructokinase 1 Pyruvate kinase Glycogen synthesis Fuel storage Glycogen synthase Pentose pathway NADPH and 5-C sugars production Glucose 6-phosphate dehydrogenase Tricarboxylic acid cycle Oxidizes pyruvate to generate NADH and FADH2 Pyruvate dehydrogenase complex α-ketoglutarate dehydrogenase Isocitrate dehydrogenase Cholesterol synthesis Produces steroid hormone precursor HMG-CoA reductase Fatty acid synthesis Produces free fatty acids and transported as VLDL for fuel storage in periphral tissues Acetyl-CoA carboxylase Urea cycle Nitrogen disposal Carbamoyl phosphate synthetase I TABLE NO. 2 SUMMARY OF METABOLISM DURING THE FED STATE
FASTED STATE METABOLISM • Approximately two hours after a meal, the decrease in serum glucose levels will lead to decreased insulin production in the pancreas. At this point in fasted state metabolism, the insulin to glucagon ratio becomes less than 1 (insulin low; glucagon high) with an additional increase of cortisol and epinephrine. Under these conditions tissues will transition to utilizing alternative fuels for energy as a means of maintaining glucose homeostasis. Fasted state metabolism will have limited impact on the oxidation of glucose by the brain and red blood cells, but it will lead to an increase in fatty acid oxidation by both the skeletal muscle and the liver (figure 3.6). The fatty acids oxidized by these tissues are released through the process of epinephrine-mediated lipolysis from the adipose. In the fasted state, the liver will primarily release glucose using both gluconeogenesis and glycogenolysis for the maintenance of blood glucose. • Liver metabolism • The primary role of the liver in the fasted state is to synthesize and release glucose. To facilitate this task, the liver will use circulating free fatty acids as the primary fuel source to generate energy (ATP) for these homeostatic processes. • 1.Glycogenolysis. Hepatic glycogenolysis provides glucose that is released into the bloodstream to maintain blood glucose and provide an oxidizable substrate for the brain and RBCs . • 2.Gluconeogenesis. This is an anabolic process that synthesizes glucose from lactate, amino acids, or glycerol. This process is heavily reliant on the ATP generated from β -oxidation. The glucose produced is released into the bloodstream to maintain blood glucose and provide an oxidizable substrate for the brain and RBCs.
3.Fatty acid β -oxidation. This is the process by which free fatty acids are oxidized to produce acetyl-CoA, NADH, and FADH 2 . It is a high energy yielding process and is required to generate ATP in the fasted state. 4.Ketogenesis. This process utilizes the acetyl-CoA produced through β -oxidation to produce β - hydroxybutyrate and acetoacetate. These ketone bodies can be oxidized by peripheral tissues; the liver cannot oxidize ketone bodies. 5.Urea cycle. Cortisol initiated protein catabolism provides amino acids needed as a substrate for gluconeogenesis. In order to use the carbon skeletons (keto-acids), the amino acids must be deaminated and the ammonia is disposed of through the synthesis of urea; nitrogen will enter the urea cycle as aspartate or free ammonia. Red blood cell metabolism The red blood cell lacks mitochondria, therefore it oxidizes glucose under both fed and fasted conditions. The metabolism of this tissue remains largely unchanged. Brain metabolism The brain will oxidize glucose under most conditions with the exception of starvation states. Under normal fasting conditions, although ketones will be synthesized, the brain will not transition to utilizing them as a predominant source of fuel until extended fasting has occurred (days). Skeletal metabolism The skeletal muscle will increases uptake of fatty acids and kitones.
Fatty acid β -oxidation. This is the process by which free fatty acids are oxidized to produce acetyl-CoA, NADH, and FADH 2 (section 5.2). Oxidation of ketones. Ketone bodies taken up by the skeletal muscle can be reconverted to acetyl-CoA and oxidized in the TCA cycle (section 5.2). Protein catabolism. Cortisol-mediated protein catabolism is also active and supplies amino acids for gluconeogenesis in the liver. Adipose metabolism The most important process in the adipose tissue during the fasted state is lipolysis. Lipolysis. This process will release fatty acids from stored triacylglycerols and provides an oxidizable substrate for the skeletal muscle and liver (section 5.2 TABLE NO 3 SUMMARY TABLE OF FULES USED IN THE FASTED STATE Tissue type Fuel utilized in the fasted state Pathway providing the fuel Liver Fatty acids Lipolysis in the adipose Red blood cells Glucose Hepatic glycogenolysis and gluconeogenesis Brain Glucose Hepatic glycogenolysis and gluconeogenesis Skeletal muscle Fatty acids Lipolysis in the adipose
fig 2 overview of the fasted state
Pathway Summary Regulatory enzyme Glycogenolysis Provides glucose for maintenance of blood glucose Glycogen phosphorylase Gluconeogenesis Provides glucose for maintenance of blood glucose Glucose 6-phosphatase Fructose 1,6-biphosphatase PEPCK/pyruvate carboxylase Lipolysis Releases free fatty acids from adipose Hormone sensitive lipase Fatty acid β-oxidation Generates ATP in the fasted state Carnitine palmitoyltransferase Ketogenesis Generates ketone bodies Driven by substrate availability HMG-CoA synthase Urea cycle Nitrogen disposal Carbamoyal phosphate synthestase i TABLE 4. SUMMARY OF METABOLISM DURING THE FASTED STATE
FED VS FASTED STATE • The presence of food may affect drug absorption via a variety of mechanisms by impacting GI tract physiology, drug solubility and dissolution, and drug permeation. • For eg. lipophilic drugs often show increased systemic exposure with food, and this phenomenon is attributable to improved solubilization due to higher bile salt and lipid concentrations. • One of the frequently used approaches to assess the effect of food on oral drug absorption involves animal studies. • However, due to the fact that physiological factors are species dependent, thus complicating the prediction of food effects in humans. • One alternative to animal experiments is to simulate food effects in humans using physiologically based absorption models. • Considering that these models are built based on a prior knowledge of GI physiology in the fasted and fed states, they are able to describe the kinetics of drug transit, dissolution, and absorption on the basis of drug- specific features such as permeability, biorelevant solubility, ionization constant(s), dose, metabolism and distribution data, etc. • Biorelevant solubilities were measured in different media: simulated human gastric fluid for the fasted and fed state, simulated human intestinal fluid for the fasted, fed, and high-fat state, and simulated human colonic fluid for the upper and the lower colon.
The effect of food was simulated by changing physiological parameters and inserting the relevant solubility data into the appropriate ACAT compartments (stomach, intestine, and colon). The food effect for each drug was estimated by comparing AUC or C max between fasted, fed, and/or high- fat conditions. Predicted and observed plasma concentration- time profiles and food effects were compared for a range of doses to assess the accuracy of the simulations. The obtained results demonstrated that GI simulation using GastroPlus™ was able to correctly predict the observed plasma exposure in fasted, fed, and high-fat conditions for all six compound.
CONCLUSION The applied method was able to accurately distinguish between minor and significant food effects. Therefore, it was concluded that biorelevant solubility tests, in conjunction with physiologically based absorption modeling, can be used to predict food effects caused by solubility and dissolution rate limitations, and/or degradation. REFERENCES 1Virtual Clinical Trials: Challenges and Opportunities: Proceedings of a Workshop. Editors: National Academies of Sciences, Engineering, and Medicine; Health and Medicine Division; Board on Health Sciences Policy; Forum on Drug Discovery, Development, and Translation; Shore C, Khandekar E, Alper J, editors. 2 Computer- aided biopharmaceutical characterization: gastrointestinal absorption simulation Sandra Grbic, Jelena Parojcic, and Zorica Djuric, Department of Pharmaceutical Technology and Cosmetology, Faculty of Pharmacy, University of Belgrade
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CADD PRESENTATION ON FED VS FASTED.pptx

  • 1. A PROJECT ON A FED VS FASTED STATE SUPERVISOR; SUBMITTED BY; Dr. SUNIL KUMAR JAIN DIVYA JAISWAL M PHARM, Ph.D M PHARM(PHARMACEUTICS) (PHARMACEUTICS) 2ND SEM, DEPARTMENT OF DEPARTMENT OF PHARMACY GGV BILASPUR PHARMACY GGV BILASPUR
  • 2. CONTENT 1. INTRODUCTION 2. FED STATE METABOLISM a) insulin independent glucose uptake b) Insulin dependent glucose uptake 3. FASTED STATE METABOLISM a) Liver metabolism b) Red blood cell metabolism c) Brain metabolism d) Skeletal muscle metabolism e) Adipose metabolism 4. FED VS FASTED STATE 5. COCLUSION
  • 3. INTRODUCTION • Intermittent Fasting (Time-Restricted Eating) Fed vs. Fasted Your body is designed to smoothly transition between two different and opposing states: ‘Fed’, and ‘Fasted’. • In the fed state, insulin is elevated, and this signals your body to store excess calories in your fat cells. In the presence of insulin, the burning of fat is halted, while the body burns glucose (from your last meal) instead. • In the fasted state, insulin is low (while glucagon and growth hormone, opposing hormones to insulin, are elevated). The body starts mobilizing stored body fat from your fat cells and burning this fat for energy (instead of glucose). • FED STATE refers to the period following a meal and is characterized by levels of nutrients in the blood. There are high circulating levels of a family of simple sugar was most important being glucose. • FASTED STATE: it means exercising after having not eaten for several hours typically early in the morning when your last meal was dinner. • Glucose homeostasis is fundamental to the human body and regulated primarily by the levels of four major hormones. 1insulin 2 glucagon 3 cortisol 4 epinephrine
  • 4. FED STATE METABOILSM In the fed state, or postprandial, elevated glucose levels trigger the release of insulin from the pancreas. As insulin levels rise, there is an increase in glucose uptake, oxidation, and storage in peripheral tissues as well as increases in other anabolic pathways. Under these conditions, most tissues (liver, skeletal muscle, adipose, brain, and red blood cells) will increase glucose uptake and oxidation (table 1). Each tissue will take up glucose in the fed state using one of the glucose transporters (GLUT) known to facilitate glucose transport across the plasma membrane. This family of proteins can be broadly categorized as insulin- independent and insulin-dependent transporters. TABLE 1 SUMMARY TABLE OF FULES USED IN THE FED STATE Tissue type Fuel utilized in fed state Primary glucose transporter Liver Glucose GLUT2 (insulin-independent) Red blood cells Glucose GLUT1 (insulin-independent) Brain Glucose GLUT1 and GLUT3 (insulin- independent) Skeletal muscle Glucose GLUT4 (insulin-dependent) Adipose Glucose GLUT4 (insulin-dependent)
  • 5. INSULIN INDEPENDENT GLUCOSE UPTAKE • The brain and red blood cells will always preferentially oxidize glucose regardless of hormone levels. Consequently, both tissues have a prevalence of GLUT1 transporters on the cell membrane. • GLUT1 is present on the blood brain barrier, while GLUT3 is predominant on the brain. • GLUT1 has a lower Km (higher affinity) for glucose, ensuring glucose transport to these important tissues. Likewise, glucose uptake in the liver is also insulin-independent and is facilitated by GLUT2 transporters. The pancreas also predominantly expresses GLUT1 and is able to take up glucose in this manner. • Red blood cell metabolism • The red blood cell lacks mitochondria, therefore it oxidizes glucose under both fed and fasted conditions. Glucose can be oxidized by: • Glycolysis. Glucose is oxidized to pyruvate and converted to lactate, which will enter the Cori Cycle. (Lactate is returned to the liver and used as a substrate for gluconeogenesis.) • Pentose phosphate pathway. Glucose is initially oxidized to ribulose 5-phosphate. In addition to the production of this 5-C sugar, more importantly NADPH is produced, which is needed as a reducing agent in the red blood cell
  • 6. fig 1. overview of fed state
  • 7. Brain metabolism The brain will preferentially oxidize glucose under most conditions with the exception of starvation states. Liver metabolism In the liver, glucose is taken up in an insulin-independent manner, and the activity of the following processes increased in the fed state are summarized in table 1and 2 1.Glycolysis. Glucose will be oxidized to pyruvate, which can enter the TCA cycle after conversion to acetyl-CoA . 2.Glycogen synthesis. Glucose 6-phosphate is used to synthesize glycogen. Pentose phosphate pathway. Glucose 6-phosphate can be used to generate five-carbon sugars and NADPH. 3.Tricarboxylic acid cycle. The TCA cycle will oxidize acetyl-CoA to generate NADH, FADH 2 , and GTP. The acetyl- CoA that enters the cycle is fully oxidized and released as CO2. 4.Cholesterol synthesis. Acetyl-CoA transported to the cytosol is used to synthesize cholesterol, which can be used for many cellular process. 5.Fatty acid synthesis. Excess citrate from the TCA cycle is shuttled out of the mitochondria and cleaved into oxaloacetate (OAA) and acetyl-CoA. The cytosolic acetyl-CoA can be used for fatty acid synthesis or cholesterol synthesis (section 4.4). Ultimately fatty acid synthesis leads to VLDL synthesis and secretion. 6.Urea cycle. Depending on diet and translation needs, excess amino acids will be deaminated through transamination reactions, and the nitrogen will enter the urea cycle as aspartate or free ammonia. Excess amino acids are not stored, rather the deaminated carbon skeletons can be stored as glycogen or triacylglycerol.
  • 8. INSULIN DEPENDENT GLUCOSE UPTAKE • in contrast, the skeletal muscle and adipose tissues require insulin for glucose uptake. GLUT4 is the primary glucose transporter on these tissues, and in the absence of insulin this transporter is predominantly bound to intracellular vesicles. When the cell receives a signal (via insulin binding the insulin receptor), this cell signaling event allows the GLUT4 containing vesicles to fuse with the plasma membrane where it will facilitate glucose uptake. Skeletal muscle metabolism The skeletal muscle will increase uptake of both amino acids and glucose under fed conditions. Glycolysis. Glucose will be oxidized to pyruvate, which can enter the TCA cycle after conversion to acetyl-CoA. Protein synthesis. Amino acids will be used for protein synthesis (anabolic metabolism). Glycogen synthesis. Glucose 1-phosphate can be converted to UDP-glucose and stored as glycogen. Adipose metabolism In the adipose tissue, glucose as well as dietary fat and cholesterol (transported as chylomicrons; are taken up by the adipose tissue. Glucose has several potential fates described below, while dietary fat is stored as triacylglycerol. Glycolysis. Glucose can be oxidized to pyruvate which can enter the TCA cycle after conversion to acetyl-CoA. Pentose phosphate pathway. Glucose will be oxidized to generate NADPH needed for fatty acid synthesis. TAG synthesis. Oxidation of glucose to glycerol 3-phosphate is needed for the synthesis of triacylglycerols (TAGs).
  • 9. Pathway Summary Regulatory enzyme Glycolysis Glucose oxidation to pyruvate Glucokinase/Hexokinase Phosphofructokinase 1 Pyruvate kinase Glycogen synthesis Fuel storage Glycogen synthase Pentose pathway NADPH and 5-C sugars production Glucose 6-phosphate dehydrogenase Tricarboxylic acid cycle Oxidizes pyruvate to generate NADH and FADH2 Pyruvate dehydrogenase complex α-ketoglutarate dehydrogenase Isocitrate dehydrogenase Cholesterol synthesis Produces steroid hormone precursor HMG-CoA reductase Fatty acid synthesis Produces free fatty acids and transported as VLDL for fuel storage in periphral tissues Acetyl-CoA carboxylase Urea cycle Nitrogen disposal Carbamoyl phosphate synthetase I TABLE NO. 2 SUMMARY OF METABOLISM DURING THE FED STATE
  • 10. FASTED STATE METABOLISM • Approximately two hours after a meal, the decrease in serum glucose levels will lead to decreased insulin production in the pancreas. At this point in fasted state metabolism, the insulin to glucagon ratio becomes less than 1 (insulin low; glucagon high) with an additional increase of cortisol and epinephrine. Under these conditions tissues will transition to utilizing alternative fuels for energy as a means of maintaining glucose homeostasis. Fasted state metabolism will have limited impact on the oxidation of glucose by the brain and red blood cells, but it will lead to an increase in fatty acid oxidation by both the skeletal muscle and the liver (figure 3.6). The fatty acids oxidized by these tissues are released through the process of epinephrine-mediated lipolysis from the adipose. In the fasted state, the liver will primarily release glucose using both gluconeogenesis and glycogenolysis for the maintenance of blood glucose. • Liver metabolism • The primary role of the liver in the fasted state is to synthesize and release glucose. To facilitate this task, the liver will use circulating free fatty acids as the primary fuel source to generate energy (ATP) for these homeostatic processes. • 1.Glycogenolysis. Hepatic glycogenolysis provides glucose that is released into the bloodstream to maintain blood glucose and provide an oxidizable substrate for the brain and RBCs . • 2.Gluconeogenesis. This is an anabolic process that synthesizes glucose from lactate, amino acids, or glycerol. This process is heavily reliant on the ATP generated from β -oxidation. The glucose produced is released into the bloodstream to maintain blood glucose and provide an oxidizable substrate for the brain and RBCs.
  • 11. 3.Fatty acid β -oxidation. This is the process by which free fatty acids are oxidized to produce acetyl-CoA, NADH, and FADH 2 . It is a high energy yielding process and is required to generate ATP in the fasted state. 4.Ketogenesis. This process utilizes the acetyl-CoA produced through β -oxidation to produce β - hydroxybutyrate and acetoacetate. These ketone bodies can be oxidized by peripheral tissues; the liver cannot oxidize ketone bodies. 5.Urea cycle. Cortisol initiated protein catabolism provides amino acids needed as a substrate for gluconeogenesis. In order to use the carbon skeletons (keto-acids), the amino acids must be deaminated and the ammonia is disposed of through the synthesis of urea; nitrogen will enter the urea cycle as aspartate or free ammonia. Red blood cell metabolism The red blood cell lacks mitochondria, therefore it oxidizes glucose under both fed and fasted conditions. The metabolism of this tissue remains largely unchanged. Brain metabolism The brain will oxidize glucose under most conditions with the exception of starvation states. Under normal fasting conditions, although ketones will be synthesized, the brain will not transition to utilizing them as a predominant source of fuel until extended fasting has occurred (days). Skeletal metabolism The skeletal muscle will increases uptake of fatty acids and kitones.
  • 12. Fatty acid β -oxidation. This is the process by which free fatty acids are oxidized to produce acetyl-CoA, NADH, and FADH 2 (section 5.2). Oxidation of ketones. Ketone bodies taken up by the skeletal muscle can be reconverted to acetyl-CoA and oxidized in the TCA cycle (section 5.2). Protein catabolism. Cortisol-mediated protein catabolism is also active and supplies amino acids for gluconeogenesis in the liver. Adipose metabolism The most important process in the adipose tissue during the fasted state is lipolysis. Lipolysis. This process will release fatty acids from stored triacylglycerols and provides an oxidizable substrate for the skeletal muscle and liver (section 5.2 TABLE NO 3 SUMMARY TABLE OF FULES USED IN THE FASTED STATE Tissue type Fuel utilized in the fasted state Pathway providing the fuel Liver Fatty acids Lipolysis in the adipose Red blood cells Glucose Hepatic glycogenolysis and gluconeogenesis Brain Glucose Hepatic glycogenolysis and gluconeogenesis Skeletal muscle Fatty acids Lipolysis in the adipose
  • 13. fig 2 overview of the fasted state
  • 14. Pathway Summary Regulatory enzyme Glycogenolysis Provides glucose for maintenance of blood glucose Glycogen phosphorylase Gluconeogenesis Provides glucose for maintenance of blood glucose Glucose 6-phosphatase Fructose 1,6-biphosphatase PEPCK/pyruvate carboxylase Lipolysis Releases free fatty acids from adipose Hormone sensitive lipase Fatty acid β-oxidation Generates ATP in the fasted state Carnitine palmitoyltransferase Ketogenesis Generates ketone bodies Driven by substrate availability HMG-CoA synthase Urea cycle Nitrogen disposal Carbamoyal phosphate synthestase i TABLE 4. SUMMARY OF METABOLISM DURING THE FASTED STATE
  • 15. FED VS FASTED STATE • The presence of food may affect drug absorption via a variety of mechanisms by impacting GI tract physiology, drug solubility and dissolution, and drug permeation. • For eg. lipophilic drugs often show increased systemic exposure with food, and this phenomenon is attributable to improved solubilization due to higher bile salt and lipid concentrations. • One of the frequently used approaches to assess the effect of food on oral drug absorption involves animal studies. • However, due to the fact that physiological factors are species dependent, thus complicating the prediction of food effects in humans. • One alternative to animal experiments is to simulate food effects in humans using physiologically based absorption models. • Considering that these models are built based on a prior knowledge of GI physiology in the fasted and fed states, they are able to describe the kinetics of drug transit, dissolution, and absorption on the basis of drug- specific features such as permeability, biorelevant solubility, ionization constant(s), dose, metabolism and distribution data, etc. • Biorelevant solubilities were measured in different media: simulated human gastric fluid for the fasted and fed state, simulated human intestinal fluid for the fasted, fed, and high-fat state, and simulated human colonic fluid for the upper and the lower colon.
  • 16. The effect of food was simulated by changing physiological parameters and inserting the relevant solubility data into the appropriate ACAT compartments (stomach, intestine, and colon). The food effect for each drug was estimated by comparing AUC or C max between fasted, fed, and/or high- fat conditions. Predicted and observed plasma concentration- time profiles and food effects were compared for a range of doses to assess the accuracy of the simulations. The obtained results demonstrated that GI simulation using GastroPlus™ was able to correctly predict the observed plasma exposure in fasted, fed, and high-fat conditions for all six compound.
  • 17.
  • 18. CONCLUSION The applied method was able to accurately distinguish between minor and significant food effects. Therefore, it was concluded that biorelevant solubility tests, in conjunction with physiologically based absorption modeling, can be used to predict food effects caused by solubility and dissolution rate limitations, and/or degradation. REFERENCES 1Virtual Clinical Trials: Challenges and Opportunities: Proceedings of a Workshop. Editors: National Academies of Sciences, Engineering, and Medicine; Health and Medicine Division; Board on Health Sciences Policy; Forum on Drug Discovery, Development, and Translation; Shore C, Khandekar E, Alper J, editors. 2 Computer- aided biopharmaceutical characterization: gastrointestinal absorption simulation Sandra Grbic, Jelena Parojcic, and Zorica Djuric, Department of Pharmaceutical Technology and Cosmetology, Faculty of Pharmacy, University of Belgrade